Porter Aidan W, Vorndran Hannah E, Marciszyn Allison, Mutchler Stephanie M, Subramanya Arohan R, Kleyman Thomas R, Hendershot Linda M, Brodsky Jeffrey L, Buck Teresa M
Department of Biological Sciences, University of Pittsburgh, Pittsburgh, Pennsylvania, United States.
Division of Pediatric Nephrology, University of Pittsburgh, Pittsburgh, Pennsylvania, United States.
Am J Physiol Renal Physiol. 2025 Feb 1;328(2):F173-F189. doi: 10.1152/ajprenal.00192.2024. Epub 2024 Nov 18.
The maintenance of fluid and electrolyte homeostasis by the kidney requires proper folding and trafficking of ion channels and transporters in kidney epithelia. Each of these processes requires a specific subset of a diverse class of proteins termed molecular chaperones. One such chaperone is GRP170, which is an Hsp70-like, endoplasmic reticulum (ER)-localized chaperone that plays roles in protein quality control and protein folding in the ER. We previously determined that loss of GRP170 in the mouse nephron leads to hypovolemia, electrolyte imbalance, and rapid weight loss. In addition, GRP170-deficient mice develop an acute kidney injury (AKI)-like phenotype, typified by tubular injury, elevation of kidney injury markers, and induction of the unfolded protein response (UPR). By using an inducible GRP170 knockout cellular model, we confirmed that GRP170 depletion induces the UPR, triggers apoptosis, and disrupts protein homeostasis. Based on these data, we hypothesized that UPR induction underlies hyponatremia and volume depletion in these rodents and that these and other phenotypes might be rectified by sodium supplementation. To test this hypothesis, control and GRP170 tubule-specific knockout mice were provided a diet containing 8% sodium chloride. We discovered that sodium supplementation improved electrolyte imbalance and kidney injury markers in a sex-specific manner but was unable to restore weight or tubule integrity. These results are consistent with UPR induction contributing to the kidney injury phenotype in the nephron-specific GR170 knockout model and indicate that GRP170 function in kidney epithelia is essential to both maintain electrolyte balance and ER homeostasis. Loss of the endoplasmic reticulum chaperone, GRP170, results in widespread kidney injury and induction of the unfolded protein response (UPR). We now show that sodium supplementation is able to at least partially restore electrolyte imbalance and reduce kidney injury markers in a sex-dependent manner.
肾脏对液体和电解质平衡的维持需要肾脏上皮细胞中离子通道和转运蛋白的正确折叠及运输。这些过程中的每一个都需要一类被称为分子伴侣的蛋白质中的特定子集。其中一种伴侣蛋白是GRP170,它是一种类似Hsp70的、定位于内质网(ER)的伴侣蛋白,在ER的蛋白质质量控制和蛋白质折叠中发挥作用。我们之前确定,小鼠肾单位中GRP170的缺失会导致血容量不足、电解质失衡和体重快速下降。此外,GRP170缺陷小鼠会出现急性肾损伤(AKI)样表型,其特征为肾小管损伤、肾损伤标志物升高以及未折叠蛋白反应(UPR)的诱导。通过使用诱导性GRP170敲除细胞模型,我们证实GRP170的缺失会诱导UPR、触发细胞凋亡并破坏蛋白质稳态。基于这些数据,我们推测UPR的诱导是这些啮齿动物低钠血症和容量耗竭的基础,并且补充钠可能会纠正这些以及其他表型。为了验证这一假设,给对照小鼠和GRP170肾小管特异性敲除小鼠提供含8%氯化钠的饮食。我们发现补充钠以性别特异性方式改善了电解质失衡和肾损伤标志物,但无法恢复体重或肾小管完整性。这些结果与UPR诱导导致肾单位特异性GR170敲除模型中的肾损伤表型一致,并表明GRP170在肾脏上皮细胞中的功能对于维持电解质平衡和ER稳态至关重要。内质网伴侣蛋白GRP170的缺失会导致广泛的肾损伤和未折叠蛋白反应(UPR)的诱导。我们现在表明,补充钠能够至少部分恢复电解质失衡,并以性别依赖的方式降低肾损伤标志物。
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